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培养的大鼠气管上皮细胞中致癌物诱导的早期癌前变化频率高。

High frequency of carcinogen-induced early, preneoplastic changes in rat tracheal epithelial cells in culture.

作者信息

Thomassen D G, Gray T E, Mass M J, Barrett J C

出版信息

Cancer Res. 1983 Dec;43(12 Pt 1):5956-63.

PMID:6640541
Abstract

To study the mechanisms of carcinogenesis, we have developed a system that uses normal cells from an environmentally and epidemiologically relevant tissue, respiratory epithelium. The induction of preneoplastic variants of epithelial cells in culture was quantitated on a per-cell basis following exposure of rat tracheal epithelial (RTE) cells in vitro to the direct-acting carcinogen N-methyl-N'-nitro-N-nitrosoguanidine (MNNG). Following treatment of normal RTE cells, large colonies of altered cells exhibiting an enhanced growth potential under selective culture conditions were observed, while normal RTE cells ceased proliferation after several cell doublings. After further growth in culture, these altered cells acquired the ability to grow in semisolid medium and to produce squamous cell carcinomas when injected into nude mice. The induction of enhanced growth variants of RTE cells by MNNG occurred with a high frequency (greater than or equal to 2.6%/colony-forming cell). In addition, a linear dose-response curve with a slope of approximately 1 was observed when the logarithm of MNNG-induced transformation frequency was plotted versus the logarithm of MNNG dose. These results are consistent with a one-hit mechanism for induction of preneoplastic variants of RTE cells by MNNG. Similar frequencies and kinetics of induction of preneoplastic variants in other culture systems using diploid cells have been observed, suggesting a common mechanism for this early step in carcinogenesis. The RTE cell system will be useful for mechanistic studies of early as well as late changes in the development of neoplasia by epithelial cells.

摘要

为了研究致癌机制,我们开发了一种系统,该系统使用来自环境和流行病学相关组织——呼吸道上皮的正常细胞。在体外将大鼠气管上皮(RTE)细胞暴露于直接作用的致癌物N-甲基-N'-硝基-N-亚硝基胍(MNNG)后,以每个细胞为基础对培养物中上皮细胞的癌前变体诱导情况进行了定量分析。在用正常RTE细胞处理后,观察到在选择性培养条件下表现出增强生长潜力的大量改变细胞集落,而正常RTE细胞在几次细胞倍增后停止增殖。在培养中进一步生长后,这些改变的细胞获得了在半固体培养基中生长的能力,并在注射到裸鼠体内时产生鳞状细胞癌。MNNG对RTE细胞增强生长变体的诱导以高频率发生(大于或等于2.6%/集落形成细胞)。此外,当将MNNG诱导的转化频率的对数与MNNG剂量的对数作图时,观察到一条斜率约为1的线性剂量反应曲线。这些结果与MNNG诱导RTE细胞癌前变体的单 hit 机制一致。在使用二倍体细胞的其他培养系统中也观察到了类似频率和动力学的癌前变体诱导,这表明在致癌作用的这一早期步骤中存在共同机制。RTE细胞系统将有助于上皮细胞肿瘤形成发展早期和晚期变化的机制研究。

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